Kinetic Analysis of Drug–Target Interactions with PET for Characterization of Pharmacological Hysteresis

Author:

Salinas Cristian1,Weinzimmer David2,Searle Graham1,Labaree David2,Ropchan Jim2,Huang Yiyun2,Rabiner Eugenii A13,Carson Richard E2,Gunn Roger N134

Affiliation:

1. GlaxoSmithKline, Clinical Imaging Centre, Hammersmith Hospital, London, UK

2. Yale PET Center, Yale School of Medicine, New Haven, Connecticut, USA

3. Department of Medicine, Imperial College London, London, UK

4. Department of Engineering Science, University of Oxford, Oxford, UK.

Abstract

In vivo characterization of the brain pharmacokinetics of novel compounds provides important information for drug development decisions involving dose selection and the determination of administration regimes. In this context, the compound-target affinity is the key parameter to be estimated. However, if compounds exhibit a dynamic lag between plasma and target bound concentrations leading to pharmacological hysteresis, care needs to be taken to ensure the appropriate modeling approach is used so that the system is characterized correctly and that the resultant estimates of affinity are correct. This work focuses on characterizing different pharmacokinetic models that relate the plasma concentration to positron emission tomography outcomes measurements (e.g., volume of distribution and target occupancy) and their performance in estimating the true in vivo affinity. Measured (histamine H3 receptor antagonist—GSK189254) and simulated data sets enabled the investigation of different modeling approaches. An indirect pharmacokinetic-receptor occupancy model was identified as a suitable model for the calculation of affinity when a compound exhibits pharmacological hysteresis.

Publisher

SAGE Publications

Subject

Cardiology and Cardiovascular Medicine,Clinical Neurology,Neurology

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